Title of article :
Aminoimidazo[1,2-a]pyridines as a new structural class of cyclin-dependent kinase inhibitors. Part 1: Design, synthesis, and biological evaluation
Author/Authors :
Carlos Jaramillo، نويسنده , , J. Eugenio de Diego، نويسنده , , Chafiq Hamdouchi، نويسنده , , Elizabeth Collins، نويسنده , , Heather Keyser، نويسنده , , Concha Sanchez-Martinez، نويسنده , , Miriam del Prado، نويسنده , , Bryan Norman، نويسنده , , Harold B. Brooks، نويسنده , , Scott A. Watkins، نويسنده , , Charles D. Spencer، نويسنده , , Jack Alan Dempsey، نويسنده , , Bryan D. Anderson، نويسنده , , Robert M. Campbell، نويسنده , , Tellie Leggett، نويسنده , , Bharvin Patel، نويسنده , , Richard M. Schultz، نويسنده , , Manuel Juan-Espinosa، نويسنده , , Michal Vieth، نويسنده , , Faming Zhang، نويسنده , , et al.، نويسنده ,
Abstract :
We have identified a novel structural class of protein serine/threonine kinase inhibitors comprised of an aminoimidazo[1,2-a]pyridine nucleus. Compounds from this family are shown to potently inhibit cyclin-dependent kinases by competing with ATP for binding to a catalytic subunit of the protein. Structure-based design approach was used to direct this chemical scaffold toward generating potent and selective CDK2 inhibitors. The discovery of this new class of ATP-site directed protein kinase inhibitors, aminoimidazo[1,2-a]pyridines, provides the basis of new medicinal chemistry tool in search for an effective treatment of cancer and other diseases that involve protein kinase signaling pathways.
Keywords :
Cyclin-dependent kinase , Kinase.* Corresponding author. Tel.: +34 916633408 , Imidazopyridine , fax: +34 916233591 , e-mail: c.jaramillo@lilly.com , CDK
